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β-Blockers have differential effects on the murine asthma phenotype.

Authors :
Thanawala VJ
Valdez DJ
Joshi R
Forkuo GS
Parra S
Knoll BJ
Bouvier M
Leff P
Bond RA
Source :
British journal of pharmacology [Br J Pharmacol] 2015 Oct; Vol. 172 (20), pp. 4833-46. Date of Electronic Publication: 2015 Oct 13.
Publication Year :
2015

Abstract

Background and Purpose: Our previous studies have shown the β2 -adrenoceptor and its endogenous ligand, adrenaline, are required for development of the asthma phenotype in murine asthma models. Chronic administration of some, but not other, β-blockers attenuated the asthma phenotype and led us to hypothesize that biased signalling was the basis of their differential effects, experimentally and clinically.<br />Experimental Approach: We used mice with no detectable systemic adrenaline (PNMT(-/-) ) and wild-type (WT) mice to study the effects of four β-blockers, alprenolol, carvedilol, propranolol and nadolol, in an ovalbumin sensitization and challenge (Ova S/C) murine model of asthma. The parameters measured were inflammatory cell infiltration, mucous metaplasia and airway hyperresponsiveness. To interpret the pharmacological action of these ligands quantitatively, we conducted computer simulations of three-state models of receptor activation.<br />Key Results: Ova S/C PNMT(-/-) mice do not develop an asthma phenotype. Here, we showed that administration of alprenolol, carvedilol or propranolol in the absence of interference from adrenaline using Ova S/C PNMT(-/-) mice resulted in the development of an asthma phenotype, whereas nadolol had no effect. Ova S/C WT mice did develop an asthma phenotype, and administration of alprenolol, propranolol and carvedilol had no effect on the asthma phenotype. However, nadolol prevented development of the asthma phenotype in Ova S/C WT mice. Computer simulations of these four ligands were consistent with the isolated three-state receptor model.<br />Conclusion and Implications: β-Blockers have different effects on the murine asthma phenotype that correlate with reported differences in activation or inhibition of downstream β2 -adrenoceptor signalling pathways.<br /> (© 2015 The British Pharmacological Society.)

Details

Language :
English
ISSN :
1476-5381
Volume :
172
Issue :
20
Database :
MEDLINE
Journal :
British journal of pharmacology
Publication Type :
Academic Journal
Accession number :
26211486
Full Text :
https://doi.org/10.1111/bph.13253